| Literature DB >> 34560251 |
Érica Aparecida de Oliveira1, Jagat Chauhan2, Julia Rezende da Silva3, Larissa Anastacio da Costa Carvalho3, Diogo Dias2, Danielle Gonçalves de Carvalho4, Luis Roberto Masao Watanabe3, Vito W Rebecca5, Gordon Mills6, Yiling Lu7, Aloisio Souza Felipe da Silva8, Márcia Edilaine Lopes Consolaro9, Meenhard Herlyn10, Patricia A Possik4, Colin R Goding2, Silvya Stuchi Maria-Engler11.
Abstract
In melanomas, therapy resistance can arise due to a combination of genetic, epigenetic and phenotypic mechanisms. Due to its crucial role in DNA supercoil relaxation, TOP1 is often considered an essential chemotherapeutic target in cancer. However, how TOP1 expression and activity might differ in therapy sensitive versus resistant cell types is unknown. Here we show that TOP1 expression is increased in metastatic melanoma and correlates with an invasive gene expression signature. More specifically, TOP1 expression is highest in cells with the lowest expression of MITF, a key regulator of melanoma biology. Notably, TOP1 and DNA Single-Strand Break Repair genes are downregulated in BRAFi- and BRAFi/MEKi-resistant cells and TOP1 inhibition decreases invasion markers only in BRAFi/MEKi-resistant cells. Thus, we show three different phenotypes related to TOP1 levels: i) non-malignant cells with low TOP1 levels; ii) metastatic cells with high TOP1 levels and high invasiveness; and iii) BRAFi- and BRAFi/MEKi-resistant cells with low TOP1 levels and high invasiveness. Together, these results highlight the potential role of TOP1 in melanoma progression and resistance.Entities:
Keywords: MITF; Melanoma; Resistance; TOP1; Topotecan
Mesh:
Substances:
Year: 2021 PMID: 34560251 PMCID: PMC8729257 DOI: 10.1016/j.phrs.2021.105911
Source DB: PubMed Journal: Pharmacol Res ISSN: 1043-6618 Impact factor: 7.658